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  • Oxford University Press  (12,458)
  • International Union of Crystallography  (5,877)
  • Annual Reviews
  • Periodicals Archive Online (PAO)
  • 1995-1999  (19,574)
  • 1980-1984
  • 1945-1949  (3,021)
  • 1997  (8,296)
  • 1996  (11,278)
  • 1948  (1,992)
  • 1945  (1,029)
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  • 1995-1999  (19,574)
  • 1980-1984
  • 1945-1949  (3,021)
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  • 1
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    Palo Alto, Calif. : Annual Reviews
    Annual Review of Biophysics and Biomolecular Structure 25 (1996), S. 55-78 
    ISSN: 1056-8700
    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
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  • 2
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    Palo Alto, Calif. : Annual Reviews
    Annual Review of Biophysics and Biomolecular Structure 25 (1996), S. 113-136 
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    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
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  • 3
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    Palo Alto, Calif. : Annual Reviews
    Annual Review of Biophysics and Biomolecular Structure 25 (1996), S. 163-195 
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    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
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  • 4
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    Palo Alto, Calif. : Annual Reviews
    Annual Review of Biophysics and Biomolecular Structure 25 (1996), S. 231-258 
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    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
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  • 5
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    Palo Alto, Calif. : Annual Reviews
    Annual Review of Biophysics and Biomolecular Structure 25 (1996), S. 259-286 
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    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
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  • 6
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    Palo Alto, Calif. : Annual Reviews
    Annual Review of Biophysics and Biomolecular Structure 25 (1996), S. 197-229 
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  • 7
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    Palo Alto, Calif. : Annual Reviews
    Annual Review of Biophysics and Biomolecular Structure 25 (1996), S. 287-314 
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    Palo Alto, Calif. : Annual Reviews
    Annual Review of Biophysics and Biomolecular Structure 25 (1996), S. 315-342 
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  • 9
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    Palo Alto, Calif. : Annual Reviews
    Annual Review of Biophysics and Biomolecular Structure 25 (1996), S. 367-394 
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    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
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  • 10
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    Palo Alto, Calif. : Annual Reviews
    Annual Review of Biophysics and Biomolecular Structure 25 (1996), S. 431-459 
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  • 11
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    Palo Alto, Calif. : Annual Reviews
    Annual Review of Biophysics and Biomolecular Structure 25 (1996), S. 395-429 
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  • 12
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    Palo Alto, Calif. : Annual Reviews
    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 1-25 
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  • 13
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 27-45 
    ISSN: 1056-8700
    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
    Topics: Biology , Physics
    Notes: Abstract The scope and utility of phage display is reviewed with emphasis on medical applications and structure-based ligand and drug design, from literature mostly after 1994. General principles by which phage-displayed peptides achieve affinity and selectivity for targets are described, along with selected structural or mechanistic studies of the binding of peptides or proteins discovered or engineered by phage display. Such engineered proteins whose wild-type or mutant crystal or 2D-NMR structures yield insight about the basis for enhanced affinity or altered specificity include antibodies, zinc fingers, human growth hormone, protein A, and atrial natriuretic peptide. Structures of complexes of de novo phage-discovered peptide ligands with targets such as the Src SH3 domain, streptavidin, and erythropoietin receptor reveal the structural basis for receptor-peptide recognition in these systems.
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  • 14
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 83-112 
    ISSN: 1056-8700
    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
    Topics: Biology , Physics
    Notes: Abstract Chromatin structure is now believed to be dynamic and intimately related with cellular processes such as transcription. Over the past few years, high-resolution structures for the histones have become available. These structures and their implications for nucleosome organization are reviewed here.
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  • 15
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 113-137 
    ISSN: 1056-8700
    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
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    Notes: Abstract The evidence showing that the self-assembly of complex RNAs occurs in discrete transitions, each relating to the folding of sub-systems of increasing size and complexity starting from a state with most of the secondary structure, is reviewed. The reciprocal influence of the concentration of magnesium ions and nucleotide mutations on tertiary structure is analyzed. Several observations demonstrate that detrimental mutations can be rescued by high magnesium concentrations, while stabilizing mutations lead to a lesser dependence on magnesium ion concentration. Recent data point to the central controlling and monitoring roles of RNA-binding proteins that can bind to the different folding stages, either before full establishment of the secondary structure or at the molten globule state before the cooperative transition to the final three-dimensional structure.
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  • 16
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 139-156 
    ISSN: 1056-8700
    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
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    Notes: Abstract One of the fundamental properties of the RNA helix is its intrinsic resistance to bend- or twist-deformations. Results of a variety of physical measurements point to a persistence length of 700-800 A for double-stranded RNA in the presence of magnesium cations, approximately 1.5-2.0-fold larger than the corresponding value for DNA. Although helix flexibility represents an important, quantifiable measure of the forces of interaction within the helix, it must also be considered in describing conformational variation of nonhelix elements (e.g. internal loops, branches), since the latter always reflect the properties of the flanking helices; that is, such elements are never completely rigid. For one important element of tertiary structure, namely, the core of yeast tRNAPhe, the above consideration has led to the conclusion that the core is not substantially more flexible than an equivalent length of pure helix.
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 157-179 
    ISSN: 1056-8700
    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
    Topics: Biology , Physics
    Notes: Abstract Phospholamban is a 52-amino-acid protein that assembles into a pentamer in sarcoplasmic reticulum membranes. The protein has a role in the regulation of the resident calcium ATPase through an inhibitory association that can be reversed by phosphorylation. The phosphorylation of phospholamban is initiated by beta-adrenergic stimulation, identifying phospholamban as an important component in the stimulation of cardiac activity by beta-agonists. It is this role of phospholamban that has motivated studies in recent decades. There is evidence that phospholamban may also function as a Ca2+-selective ion channel. The structural properties of phospholamban have been studied by mutagenesis, modeling, and spectroscopy, resulting in a new view of the organization of this key molecule in membranes.
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  • 18
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    Palo Alto, Calif. : Annual Reviews
    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 181-222 
    ISSN: 1056-8700
    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
    Topics: Biology , Physics
    Notes: Abstract Innovative algorithms have been developed during the past decade for simulating Newtonian physics for macromolecules. A major goal is alleviation of the severe requirement that the integration timestep be small enough to resolve the fastest components of the motion and thus guarantee numerical stability. This timestep problem is challenging if strictly faster methods with the same all-atom resolution at small timesteps are sought. Mathematical techniques that have worked well in other multiple-timescale contexts-where the fast motions are rapidly decaying or largely decoupled from others-have not been as successful for biomolecules, where vibrational coupling is strong. This review examines general issues that limit the timestep and describes available methods (constrained, reduced-variable, implicit, symplecttic, multiple-timestep, and normal-mode-based schemes). A section compares results of selected integrators for a model dipeptide, assessing physical and numerical performance. Included is our dual timestep method LN, which relies on an approximate linearization of the equations of motion every Deltat interval (5 fs or less), the solution of which is obtained by explicit integration at the inner timestep Deltatau (e.g., 0.5 fs). LN is computationally competitive, providing 4-5 speedup factors, and results are in good agreement, in comparison to 0.5 fs trajectories. These collective algorithmic efforts help fill the gap between the time range that can be simulated and the timespans of major biological interest (milliseconds and longer). Still, only a hierarchy of models and methods, along with experimentational improvements, will ultimately give theoretical modeling the status of partner with experiment.
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  • 19
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 223-258 
    ISSN: 1056-8700
    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
    Topics: Biology , Physics
    Notes: Abstract Two sensory rhodopsins (SRI and SRII) mediate color-sensitive phototaxis responses in halobacteria. These seven-helix receptor proteins, structurally and functionally similar to animal visual pigments, couple retinal photoisomerization to receptor activation and are complexed with membrane-embedded transducer proteins (HtrI and HtrII) that modulate a cytoplasmic phosphorylation cascade controlling the flagellar motor. The Htr proteins resemble the chemotaxis transducers from Escherichia coli. The SR-Htr signaling complexes allow studies of the biophysical chemistry of signal generation and relay, from the photobiophysics of initial excitation of the receptors to the final output at the level of the flagellar motor switch, revealing fundamental principles of sensory transduction and more broadly the nature of dynamic interactions between membrane proteins. We review here recent advances that have led to new insights into the molecular mechanism of signaling by these membrane complexes.
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  • 20
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 259-288 
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    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
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    Notes: Abstract A characteristic feature of cellular signal transduction pathways in eukaryotes is the separation of catalysis from target recognition. Several modular domains that recognize short peptide sequences and target signaling proteins to these sequences have been identified. The structural bases of the specificities of recognition by SH2, SH3, and PTB domains have been elucidated by X-ray crystallography and NMR, and these results are reviewed here. In addition, the mechanism of cooperative interactions between these domains is discussed.
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  • 21
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 357-371 
    ISSN: 1056-8700
    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
    Topics: Biology , Physics
    Notes: Abstract Zinc-finger domains are small metal-binding modules that are found in a wide range of gene regulatory proteins. Peptides corresponding to these domains have provided valuable model systems for examining a number of biophysical parameters entirely unrelated to their nucleic acid binding properties. These include the chemical basis for metal-ion affinity and selectivity, thermodynamic properties related to hydrophobic packing and beta-sheet propensities, and constraints on the generation of ligand-binding and potential catalytic sites. These studies have laid the foundation for applications such as the generation of optically detected zinc probes and the design of metal-binding peptides and proteins with desired spectroscopic and chemical properties.
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  • 22
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 327-355 
    ISSN: 1056-8700
    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
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    Notes: Abstract Over the past two decades, nanosecond absorption and vibrational spectroscopies have developed into powerful tools for monitoring the secondary, tertiary, and quaternary structural relaxations of biological macromolecules under near-physiological conditions of solvent and temperature. Observed through such methods, the dynamic response of a biomolecule to photoinitiated excursions from equilibrium can reveal valuable information about the structure-function relationship, information beyond that obtained from the static structures provided by X-ray crystallography, nuclear magnetic resonance spectroscopy, and other steady-state methods. Most recently, the development of ultra-sensitive polarization techniques for absorption spectroscopy has greatly enhanced the amount of time-resolved structural information that can be obtained from the broadened electronic spectra of biomolecules. This review examines nanosecond absorption, vibrational, and polarized absorption methods, and their applications to protein function and folding, emphasizing the complementary nature of information obtained from electronic and vibrational spectra measured on the nanosecond time scale.
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 289-325 
    ISSN: 1056-8700
    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
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    Notes: Abstract Eukaryotes have three distinct RNA polymerases that catalyze transcription of nuclear genes. RNA polymerase II is responsible for transcribing nuclear genes encoding the messenger RNAs and several small nuclear RNAs. Like RNA polymerases I and III, polymerase II cannot recognize its target promoter directly and initiate transcription without accessory factors. Instead, this large multisubunit enzyme relies on general transcription factors and transcriptional activators and coactivators to regulate transcription from class II promoters. X-ray crystallography and nuclear magnetic resonance spectroscopy have been used to study complexes of general transcription factors and transcriptional activators with their specific DNA targets. This work has provided important structural insights into transcription initiation by polymerase II and the more general problem of DNA sequence recognition.
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 47-82 
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    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
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    Notes: Abstract Researchers have made good progress in unraveling the molecular mechanisms of excitation-contraction (EC) coupling in striated muscle. Despite this progress, paradoxes abound. In skeletal muscle, the existence of a mechanical coupling between membrane charge movement and activation of sarcoplasmic reticulum (SR) release channels is essentially established, but the contribution of Ca2+-induced Ca2+ release (CICR) to the transient and steady-state components of Ca2+ release remains controversial. In cardiac muscle, the role of CICR as the primary mechanism of EC coupling is well established, but the stability and tight coupling between membrane Ca2+ current and release are paradoxical. Answers may lie in microdomain issues, and in the examination of discrete elementary release events, although quantitative treatments are needed. This review explores the theoretical and experimental methods used and the observations made in the study of microdomain Ca2+.
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 373-399 
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    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
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    Notes: Abstract Measurements of trajectories of individual proteins or lipids in the plasma membrane of cells show a variety of types of motion. Brownian motion is observed, but many of the particles undergo non-Brownian motion, including directed motion, confined motion, and anomalous diffusion. The variety of motion leads to significant effects on the kinetics of reactions among membrane-bound species and requires a revision of existing views of membrane structure and dynamics.
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 495-540 
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    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
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    Notes: Abstract This review focuses on the recent advances in EPR spectroscopy as they are applied both to photoinduced electron transfer in the photosynthetic apparatus and to biomimetic systems. The review deals with time-resolved direct-detection cw and pulsed EPR and ENDOR methods, both at conventional bands [X-(9.5 GHz), K-(24 GHz), and Q-(35 GHz)] and at high frequency bands (W-band, 95 GHz, and even highter frequency bands). EPR studies on photosynthetic and model systems in their doublet, triplet and radical pair states are surveyed, including their static and dynamic properties. Applications of time-resolved EPR in studying photoinduced electron and energy transfer in isotropic and anisotropic environments, and the concepts of electron spin polarization and magnetic field effects in photochemical reactions are also reviewed.
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 541-566 
    ISSN: 1056-8700
    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
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    Notes: Abstract Surface plasmon resonance biosensors have become increasingly popular for the qualitative and quantitative characterization of the specific binding of a mobile reactant to a binding partner immobilized on the sensor surface. This article reviews the use of this new technique to measure the binding affinities and the kinetic constants of reversible interactions between biological macromolecules. Immobilization techniques, the most commonly employed experimental strategies, and various analytical approaches are summarized. In recent years, several sources of potential artifacts have been identified: immobilization of the binding partner, steric hindrance of binding to adjacent binding sites at the sensor surface, and finite rate of mass transport of the mobile reactant to the sensor surface. Described here is the influence of these artifacts on the measured binding kinetics and equilibria, together with suggested control experiments.
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 597-627 
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    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
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    Notes: Abstract Analysis of the structures in the Protein Databank, released in June 1996, shows that the number of different protein folds, i.e. the number of different arrangements of major secondary structures and/or chain topologies, is 327. Of these folds, approximately 25% belong to the all-alpha class, 20% belong to the all-beta class, 30% belong to the alpha/beta class, and 25% belong to the alpha + beta class. We describe the types of folds now known for the all-beta and all-alpha classes, emphasizing those that have been discovered recently. Detailed theories for the physical determinants of the structures of most of these folds now exist, and these are reviewed.
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    Annual Review of Cell and Developmental Biology 12 (1996), S. 1-26 
    ISSN: 1081-0706
    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
    Topics: Biology , Medicine
    Notes: Abstract Most chloroplast proteins are nuclear encoded, synthesized as larger precursor proteins in the cytosol, posttranslationally imported into the organelle, and routed to one of six different compartments. Import across the outer and inner envelope membranes into the stroma is the major means for entry of proteins destined for the stroma, the thylakoid membrane, and the thylakoid lumen. Recent investigations have identified several unique protein components of the envelope translocation machinery. These include two GTP-binding proteins that appear to participate in the early events of import and probably regulate precursor recognition and advancement into the translocon. Localization of imported precursor proteins to the thylakoid membrane and thylakoid lumen is accomplished by four distinct mechanisms; two are homologous to bacterial and endoplasmic reticulum protein transport systems, one appears unique, and the last may be a spontaneous mechanism. Thus chloroplast protein targeting is a unique and surprisingly complex process. The presence of GTP-binding proteins in the envelope translocation machinery indicates a different precursor recognition process than is present in mitochondria. Mechanisms for thylakoid protein localization are in part derived from the prokaryotic endosymbiont, but are more unusual and diverse than expected.
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    Annual Review of Cell and Developmental Biology 12 (1996), S. 181-220 
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    Topics: Biology , Medicine
    Notes: Abstract Receptors for the Fc domain of immunoglobulins play an important role in immune defense. There are two well-defined functional classes of mammalian receptors. One class of receptors transports immunoglobulins across epithelial tissues to their main sites of action. This class includes the neonatal Fc receptor (FcRn), which transports immunoglobulin G (IgG), and the polymeric immunoglobulin receptor (pIgR), which transports immunoglobulin A (IgA) and immunoglobulin M (IgM). Another class of receptors present on the surfaces of effector cells triggers various biological responses upon binding antibody-antigen complexes. Of these, the IgG receptors (FcgammaR) and immunoglobulin E (IgE) receptors (FcepsilonR) are the best characterized. The biological responses elicited include antibody-dependent, cell-mediated cytotoxicity, phagocytosis, release of inflammatory mediators, and regulation of lymphocyte proliferation and differentiation. We summarize the current knowledge of the structures and functions of FcRn, pIgR, and the FcgammaR and FcepsilonRI proteins, concentrating on the interactions of the extracellular portions of these receptors with immunoglobulins.
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    Annual Review of Cell and Developmental Biology 12 (1996), S. 335-363 
    ISSN: 1081-0706
    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
    Topics: Biology , Medicine
    Notes: Abstract Peroxisome proliferator-activated receptors (PPARs) are lipid-activated transcription factors that belong to the steroid/thyroid/retinoic acid receptor superfamily. All their characterized target genes encode proteins that participate in lipid homeostasis. The recent finding that antidiabetic thiazolidinediones and adipogenic prostanoids are ligands of one of the PPARs reveals a novel signaling pathway that directly links these compounds to processes involved in glucose homeostasis and lipid metabolism including adipocyte differentiation. A detailed understanding of this pathway could designate PPARs as targets for the development of novel efficient treatments for several metabolic disorders.
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    Annual Review of Cell and Developmental Biology 12 (1996), S. 441-461 
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    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
    Topics: Biology , Medicine
    Notes: Abstract Proteins that function in transport vesicle docking are being identified at a rapid rate. So-called v- and t-SNAREs form the core of a vesicle docking complex. Additional accessory proteins are required to protect SNAREs from promiscuous binding and to deprotect SNAREs under conditions in which transport vesicle docking should occur. Because access to SNAREs must be regulated, other proteins must also contain specificity determinants to accomplish delivery of transport vesicles to their distinct and specific membrane targets.
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    Annual Review of Cell and Developmental Biology 12 (1996), S. 417-439 
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    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
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    Notes: Abstract Myosin is a highly conserved, ubiquitous protein found in all eukaryotic cells, where it provides the motor function for diverse movements such as cytokinesis, phagocytosis, and muscle contraction. All myosins contain an amino-terminal motor/head domain and a carboxy-terminal tail domain. Due to the extensive number of different molecules identified to date, myosins have been divided into seven distinct classes based on the properties of the head domain. One such class, class II myosins, consists of the conventional two-headed myosins that form filaments and are composed of two myosin heavy chain (MYH) subunits and four myosin light chain subunits. The MYH subunit contains the ATPase activity providing energy that is the driving force for contractile processes mentioned above, and numerous MYH isoforms exist in vertebrates to carry out this function. The MYHs involved in striated muscle contraction in mammals are the focus of the current review. The genetics, molecular biology, and biochemical properties of mammalian MYHs are discussed below. MYH gene expression patterns in developing and adult striated muscles are described in detail, as are studies of regulation of MYH genes in the heart. The discovery that mutant MYH isoforms have a causal role in the human disease familial hypertrophic cardiomyopathy (FHC) has implemented structure/function investigations of MYHs. The regulation of MYH genes expressed in skeletal muscle and the potential functional implications that distinct MYH isoforms may have on muscle physiology are addressed.
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    Annual Review of Cell and Developmental Biology 12 (1996), S. 697-715 
    ISSN: 1081-0706
    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
    Topics: Biology , Medicine
    Notes: Abstract Proteins that contain the Arg-Gly-Asp (RGD) attachment site, together with the integrins that serve as receptors for them, constitute a major recognition system for cell adhesion. The RGD sequence is the cell attachment site of a large number of adhesive extracellular matrix, blood, and cell surface proteins, and nearly half of the over 20 known integrins recognize this sequence in their adhesion protein ligands. Some other integrins bind to related sequences in their ligands. The integrin-binding activity of adhesion proteins can be reproduced by short synthetic peptides containing the RGD sequence. Such peptides promote cell adhesion when insolubilized onto a surface, and inhibit it when presented to cells in solution. Reagents that bind selectively to only one or a few of the RGD-directed integrins can be designed by cyclizing peptides with selected sequences around the RGD and by synthesizing RGD mimics. As the integrin-mediated cell attachment influences and regulates cell migration, growth, differentiation, and apoptosis, the RGD peptides and mimics can be used to probe integrin functions in various biological systems. Drug design based on the RGD structure may provide new treatments for diseases such as thrombosis, osteoporosis, and cancer.
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    Annual Review of Cell and Developmental Biology 13 (1997), S. 1-23 
    ISSN: 1081-0706
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    Notes: Abstract Transcriptional regulation is important in all eukaryotic organisms for cell growth, development, and responses to environmental change. Saccharomyces cerevisiae, or bakers' yeast, has provided a powerful system for genetic analysis of transcriptional regulation, and findings from the study of this model system have proven broadly applicable to higher organisms. Transcriptional regulation requires the interactions of regulatory proteins with various components of the transcription machinery. Recently, genetic analysis of a diverse set of transcriptional regulatory responses has converged with studies of the function of the RNA polymerase II carboxy-terminal domain (CTD) to reveal regulatory roles for proteins associated with the CTD. These proteins, designated Srb/mediator proteins, are broadly involved in both positive and negative regulatory responses in vivo. This review focuses on the connections between genetic analysis of transcriptional regulation and the functions of the Srb/mediator proteins associated with the RNA polymerase II CTD.
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    Annual Review of Cell and Developmental Biology 13 (1997), S. 53-82 
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    Notes: Abstract Most animal species exhibit left-right asymmetry in their body plans and show a strong bias for one handedness over the other. The mechanism of handedness choice, recognized as an intriguing problem over a century ago, is still a mystery. However, from recent advances in understanding when and how asymmetry arises in both invertebrates and vertebrates, developmental pathways for establishment and maintenance of left-right differences are beginning to take shape, and speculations can be made on the initial choice mechanism.
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    Annual Review of Cell and Developmental Biology 13 (1997), S. 83-117 
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    Notes: Abstract The polymerization dynamics of microtubules are central to their biological functions. Polymerization dynamics allow microtubules to adopt spatial arrangements that can change rapidly in response to cellular needs and, in some cases, to perform mechanical work. Microtubules utilize the energy of GTP hydrolysis to fuel a unique polymerization mechanism termed dynamic instability. In this review, we first describe progress toward understanding the mechanism of dynamic instability of pure tubulin and then discuss the function and regulation of microtubule dynamic instability in living cells.
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    Annual Review of Cell and Developmental Biology 13 (1997), S. 25-51 
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    Notes: Abstract Mitochondria import most of their proteins from the cytosol. Dynamic protein complexes in the mitochondrial outer and inner membranes are responsible for the specific recognition and membrane translocation of preproteins. The preprotein translocase of the outer mitochondrial membrane contains several import receptors and a general import pore. The preprotein translocase of the inner membrane consists of a channel interacting with preproteins in transit and an import motor that includes the matrix heat shock protein Hsp70. Acidic patches of import components are thought to guide the import of positively charged signal sequences (acid chain hypothesis). Energy input is derived from the inner membrane potential and ATP. Proteins in the mitochondrial matrix are required for proteolytic processing and folding of imported proteins. The dynamic nature of the membrane translocase permits sorting of preproteins at distinct stages of the import pathway.
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    Annual Review of Cell and Developmental Biology 13 (1997), S. 119-146 
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    Notes: Abstract Adherens junctions are specialized forms of cadherin-based adhesive contacts important for tissue organization in developing and adult organisms. Cadherins form protein complexes with cytoplasmic proteins (catenins) that convert the specific, homophilic-binding capacity of the extracellular domain into stable cell adhesion. The extracellular domains of cadherins form parallel dimers that possess intrinsic homophilic-binding activity. Cytoplasmic interactions can influence the function of the ectodomain by a number of potential mechanisms, including redistribution of binding sites into clusters, providing cytoskeletal anchorage, and mediating physiological regulation of cadherin function. Adherens junctions are likely to serve specific, specialized functions beyond the basic adhesive process. These functions include coupling cytoskeletal force generation to strongly adherent sites on the cell surface and the regulation of intracellular signaling events.
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    Annual Review of Cell and Developmental Biology 13 (1997), S. 147-170 
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    Notes: Abstract The Drosophila ovary provides a favorable model system in which to study cellular morphogenesis. The development of a mature egg involves a syncytium of 16 germline cells and over 1000 somatically derived follicle cells. Intercellular transport, stable intercellular bridges, cell migrations, cell shape changes, and specific subcellular localization of many embryonic patterning determinants contribute to egg development and require a dynamic cytoskeleton. We discuss many of the recent genetic and cell biological studies that have led to insights into how the actin cytoskeleton is assembled and regulated during the morphogenesis of the Drosophila egg.
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    Annual Review of Cell and Developmental Biology 13 (1997), S. 333-361 
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    Notes: Abstract Notch, LIN-12, and GLP-1 are receptors that mediate a broad range of cell interactions during Drosophila and nematode development. Signaling by these receptors relies on a conserved pathway with three core components: DSL ligand, LNG receptor, and a CSL effector that links the receptor to its transcriptional response. Although key functional regions have been identified in each class of proteins, the mechanism for signal transduction is not yet understood. Diverse regulatory mechanisms influence signaling by the LIN-12/Notch pathway. Inductive signaling relies on the synthesis of ligand and receptor in distinct but neighboring cells. By contrast, lateral signaling leads to the transformation of equivalent cells that express both ligand and receptor into nonequivalent cells that express either ligand or receptor. This transformation appears to rely on regulatory feedback loops within the LIN-12/Notch pathway. In addition, the pathway can be regulated by intrinsic factors that are asymmetrically segregated during cell division or by extrinsic cues via other signaling pathways. Specificity in the pathway does not appear to reside in the particular ligand or receptor used for a given cell-cell interaction. The existence of multiple ligands and receptors may have evolved from the stringent demands placed upon the regulation of genes encoding them.
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    Annual Review of Cell and Developmental Biology 13 (1997), S. 363-393 
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    Notes: Abstract Molecules involved in cell adhesion processes are often both structurally and functionally modular, with subdomains that are members of large protein families. Recently, high-resolution structures have been determined for representative members of many of these families including fragments of integrins, cadherins, fibronectin-like domains, and immunoglobulin-like domains. These structures have enhanced our understanding of cell adhesion processes at several levels. In almost all cases, ligand-binding sites have been visualized and provide insight into how these molecules mediate biologically important interactions. Metal-binding sites have been identified and characterized, allowing assessment of the role of bound ions in cell adhesion processes. Many of these structures serve as templates for modeling homologous domains in other proteins or, when the structure of a fragment consisting of more than one domain is determined, the structure of multidomain arrays of homologous domains. Knowledge of atomic structure also allows rational design of drugs that either mimic or target specific binding sites. In many cases, high-resolution structures have revealed unexpected relationships that pose questions about the evolutionary origin of specific domains. This review briefly describes several recently determined structures of cell adhesion molecules, summarizes some of the main results of each structure, and highlights common features of different systems.
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    Annual Review of Cell and Developmental Biology 13 (1997), S. 395-424 
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    Notes: Abstract Bacteria usually divide by building a central septum across the middle of the cell. This review focuses on recent results indicating that the tubulin-like FtsZ protein plays a central role in cytokinesis as a major component of a contractile cytoskeleton. Assembly of this cytoskeletal element abutting the membrane is a key point for regulation. The characterization of FtsZ homologues in Mycoplasmas, Archaea, and chloroplasts implies that the constriction mechanism is conserved and that FtsZ can constrict in the absence of peptidoglycan synthesis. In most Eubacteria, the internal cytoskeleton must also regulate synthesis of septal peptidoglycan. The Escherichia coli septum-specific penicillin-binding protein 3 (PBP3) forms a complex with other enzymes involved in murein metabolism, suggesting a centrally located transmembrane complex capable of splicing multiple new strands of peptidoglycan into the cell wall. Important questions remain about the spatial and temporal control of bacterial division.
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    Annual Review of Cell and Developmental Biology 13 (1997), S. 425-456 
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    Notes: Abstract NCAM, L1, and DCC-immunoglobulin cell adhesion molecules (Ig CAMs)-are widely expressed during development. Many workers have dismissed a role for such molecules in the control of axonal growth and guidance because they do not show highly restricted expression patterns. Yet evidence from a number of model systems suggests all three CAMs play a role in the development of specific projections in the nervous system. For example, there is a reduction in mossy fiber tracts in the hippocampus of mice that lack NCAM, a requirement for DCC in the response of commissural neurons to a floor plate-derived chemoattractant, and a loss of corticospinal tracts in humans who carry mutations in the L1 gene. The above paradox might be explained by the observation that differential post-translational processing can modulate CAMs function and that alternative splicing can generate functionally distinct isoforms of a CAM. Activation of the FGF tyrosine kinase receptor is required for the responses stimulated by NCAM and L1, and the importance of regulated tyrosine phosphorylation for growth and guidance is underscored by the involvement of receptor tyrosine phosphatases in this process.
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    Annual Review of Cell and Developmental Biology 13 (1997), S. 513-609 
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    Notes: Abstract Src family protein tyrosine kinases are activated following engagement of many different classes of cellular receptors and participate in signaling pathways that control a diverse spectrum of receptor-induced biological activities. While several of these kinases have evolved to play distinct roles in specific receptor pathways, there is considerable redundancy in the functions of these kinases, both with respect to the receptor pathways that activate these kinases and the downstream effectors that mediate their biological activities. This chapter reviews the evidence implicating Src family kinases in specific receptor pathways and describes the mechanisms leading to their activation, the targets that interact with these kinases, and the biological events that they regulate.
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    Notes: Abstract The chemosensory pathway of bacterial chemotaxis has become a paradigm for the two-component superfamily of receptor-regulated phosphorylation pathways. This simple pathway illustrates many of the fundamental principles and unanswered questions in the field of signaling biology. A molecular description of pathway function has progressed rapidly because it is accessible to diverse structural, biochemical, and genetic approaches. As a result, structures are emerging for most of the pathway elements, biochemical studies are elucidating the mechanisms of key signaling events, and genetic methods are revealing the intermolecular interactions that transmit information between components. Recent advances include (a) the first molecular picture of a conformational transmembrane signal in a cell surface receptor, (b) four new structures of kinase domains and adaptation enzymes, and (c) significant new insights into the mechanisms of receptor-mediated kinase regulation, receptor adaptation, and the phospho-activation of signaling proteins. Overall, the chemosensory pathway and the propulsion system it regulates provide an ideal system in which to probe molecular principles underlying complex cellular signaling and behavior.
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    Annual Review of Cell and Developmental Biology 13 (1997), S. 611-667 
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    Notes: Abstract The organizer is formed in an equatorial sector of the blastula stage amphibian embryo by cells that have responded to two maternal agents: a general meso-endoderm inducer (involving the TFG-beta signaling pathway) and a dorsal modifier (probably involving the Wnt signaling pathway). The meso-endoderm inducer is secreted by most vegetal cells, those containing maternal materials that had been localized in the vegetal hemisphere of the oocyte during oogenesis. As a consequence of the inducer's distribution and action, the competence domains of prospective ectoderm, mesoderm, and endoderm are established in an animal-to-vegetal order in the blastula. The dorsal modifier signal is secreted by a sector of cells of the animal and vegetal hemispheres on one side of the blastula. These cells contain maternal materials transported there in the first cell cycle from the vegetal pole of the egg along microtubules aligned by cortical rotation. The Nieuwkoop center is the region of blastula cells secreting both maternal signals, and hence specifying the organizer in an equatorial sector. Final steps of organizer formation at the late blastula or early gastrula stage may involve locally secreted zygotic signals as well. At the gastrula stage, the organizer secretes a variety of zygotic proteins that act as antagonists to various members of the BMP and Wnt families of ligands, which are secreted by cells of the competence domains surrounding the organizer. BMPs and Wnts favor ventral development, and cells near the organizer are protected from these agents by the organizer's inducers. The nearby cells are derepressed in their inherent capacity for dorsal development, which is apparent in the neural induction of the ectoderm, dorsalization of the mesoderm, and anteriorization of the endoderm. The organizer also engages in extensive specialized morphogenesis, which brings it within range of responsive cell groups. It also self-differentiates to a variety of axial tissues of the body.
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    Annual Review of Astronomy and Astrophysics 34 (1996), S. 35-73 
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    Topics: Physics
    Notes: Abstract Two types of flows dominate the large-scale structure of the solar wind: corotating flows and transient disturbances. Corotating flows are associated with spatial variability in the coronal expansion and solar rotation, whereas transient disturbances are associated with episodic ejections of material into interplanetary space from coronal regions not previously participating in the solar wind expansion. Ulysses' recent epic journey over the poles of the Sun has provided new insights on the three-dimensional nature of both corotating flows and transient disturbances in the solar wind and their evolution with heliocentric distance and latitude. This paper provides a simple physical description of the origins and dynamics of both of these types of solar wind flows, highlighting new understanding gained from the unique Ulysses high-latitude observations.
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    Annual Review of Astronomy and Astrophysics 34 (1996), S. 207-240 
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    Notes: Abstract We summarize the properties of FU Orionis variables, and show how accretion disk models simply explain many peculiarities of these objects. FU Ori systems demonstrate that disk accretion in early stellar evolution is highly episodic, varying from ~ 10-7 yr-1 in the low (T Tauri) state to 10-4 yr-1 in the high (FU Ori) state. This variability in mass accretion is matched by a corresponding variability in mass ejection, with mass loss rates reaching ~ 10-1 of the mass accretion rates in outburst. It appears that the FU Ori phenomenon is restricted to early phases of stellar evolution, probably with infall still occuring to the disk, which may help drive repetitive outbursts. Thermal instabilities are a promising way to produce FU Ori disk outbursts, although many uncertainties remain in the theory; triggering by interactions with companion stars on eccentric orbits may also play a role.
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    Annual Review of Astronomy and Astrophysics 34 (1996), S. 383-418 
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    Topics: Physics
    Notes: Abstract In most space environments, dust particles are exposed to plasmas and UV radiation and, consequently, carry electrostatic charges. Their motion is influenced by electric and magnetic fields in addition to gravity, drag, and radiation pressure. On the surface of the Moon, in planetary rings, or at comets, for example, electromagnetic forces can shape the spatial and size distribution of micron-sized charged dust particles. The dynamics of small charged dust particles can be surprisingly complex, leading to levitation, rapid transport, energization and ejection, capture, and the formation of new planetary rings. This review briefly discusses the most important processes that determine the charge state of dust particles immersed in plasmas and the resulting dynamics on exposed dusty surfaces and in planetary magnetospheres.
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    Annual Review of Astronomy and Astrophysics 34 (1996), S. 279-329 
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    Notes: Abstract The Goddard High-Resolution Spectrograph (GHRS) aboard the Hubble Space Telescope (HST) has yielded precision abundance results for a range of interstellar environments, including gas in the local medium, in the warm neutral medium, in cold diffuse clouds, and in distant halo clouds. Through GHRS studies, investigators have determined the abundances of elements such as C, N, O, Mg, Si, S, and Fe in individual interstellar clouds. These studies have provided new information about the composition of interstellar dust grains, the origin of the Galactic high-velocity cloud system, and the processes that transport gas between the disk and the halo. Precision measurements of the interstellar D to H ratio and of the abundances of r- and s-process elements have also provided fiducial reference values for cosmological and stellar evolutionary observations and theoretical models.
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    Annual Review of Astronomy and Astrophysics 34 (1996), S. 645-701 
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    Notes: Abstract The central half kiloparsec region of our Galaxy harbors a variety of phenomena unique to the central environment. This review discusses the observed structure and activity of the interstellar medium in this region in terms of its inevitable inflow toward the center of the Galactic gravitational potential well. A number of dissipative processes lead to a strong concentration of gas into a "Central Molecular Zone" of about 200-pc radius, in which the molecular medium is characterized by large densities, large velocity dispersions, high temperatures, and apparently strong magnetic fields. The physical state of the gas and the resultant star formation processes occurring in this environment are therefore quite unlike those occurring in the large-scale disk. Gas not consumed by star formation either enters a hot X ray-emitting halo and is lost as a thermally driven galactic wind or continues moving inward, probably discontinuously, through the domain of the few parsec-sized circumnuclear disks and eventually into the central parsec. There, the central radio source SgrA* currently accepts only a tiny fraction of the inflowing material, likely as a result of a limit cycle wherein the continual inflow of matter provokes star formation, which in turn can temporarily halt the inflow via mass-outflow winds.
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    Annual Review of Astronomy and Astrophysics 34 (1996), S. 749-792 
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    Notes: Abstract At luminosities above 1011 , infrared galaxies become the dominant population of extragalactic objects in the local Universe (z〈 0.3), being more numerous than optically selected starburst and Seyfert galaxies and quasi-stellar objects at comparable bolometric luminosity. The trigger for the intense infrared emission appears to be the strong interaction/merger of molecular gas-rich spirals, and the bulk of the infrared luminosity for all but the most luminous objects is due to dust heating from an intense starburst within giant molecular clouds. At the highest luminosities (Lir〉 1012 ), nearly all objects appear to be advanced mergers powered by a mixture of circumnuclear starburst and active galactic nucleus energy sources, both of which are fueled by an enormous concentration of molecular gas that has been funneled into the merger nucleus. These ultraluminous infrared galaxies may represent an important stage in the formation of quasi-stellar objects and powerful radio galaxies. They may also represent a primary stage in the formation of elliptical galaxy cores, the formation of globular clusters, and the metal enrichment of the intergalactic medium.
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    Annual Review of Astronomy and Astrophysics 35 (1997), S. xiii 
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    Annual Review of Astronomy and Astrophysics 35 (1997), S. 33-67 
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    Notes: Abstract To what extent are changes in the Earth's global environment linked with fluctuations in its primary energy source, the radiation from a variable star, the Sun? A firm scientific basis for policy making with regard to anthropogenic greenhouse warming of climate and chlorofluorocarbon depletion of ozone requires a reliable answer to this question. Reduction of the vulnerability of spacecraft operations and communications to space weather necessitates knowledge of solar induced variability in Earth's upper atmosphere. Toward these goals, solar radiation monitoring and studies of solar variability mechanisms facilitate an understanding of the sources and amplitudes of the Sun's changing radiation. Interdisciplinary studies that link these changes with a wide array of terrestrial phenomena over the longer time scales of global change and the shorter time scales of space weather address the relevance of solar radiation variability for Earth. However, although numerous associations are apparent between solar and terrestrial fluctuations, full comprehension of the physical mechanisms responsible for the many facets of radiative Sun-Earth coupling remains to be accomplished.
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    Annual Review of Astronomy and Astrophysics 35 (1997), S. 267-307 
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    Topics: Physics
    Notes: Abstract The properties of galaxies that are lower in surface brightness than the dark night sky are reviewed. There are substantial selection effects against the discovery of galaxies that are unevolved or diffuse; these systems are missing from most wide field catalogs. Low surface brightness galaxies make up a significant amount of the luminosity density of the local universe. They contribute substantial but poorly determined amounts to the census of baryons and dark matter. Low surface brightness galaxies are also relevant to the interpretation of quasar absorption lines and to the understanding of rapidly evolving galaxy populations in the more distant universe. Theories of galaxy formation and evolution must accomodate the properties of these diffuse stellar systems.
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    Annual Review of Astronomy and Astrophysics 35 (1997), S. 357-388 
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    Notes: Abstract Compact groups of galaxies have posed a number of challenging questions. Intensive observational and theoretical studies are now providing answers to many of these and, at the same time, are revealing unexpected new clues about the nature and role of these systems. Most compact groups contain a high fraction of galaxies having morphological or kinematical peculiarities, nuclear radio and infrared emission, and starburst or active galactic nuclei (AGN) activity. They contain large quantities of diffuse gas and are dynamically dominated by dark matter. They most likely form as subsystems within looser associations and evolve by gravitational processes. Strong galaxy interactions result and merging is expected to lead to the ultimate demise of the group. Compact groups are surprisingly numerous and may play a significant role in galaxy evolution.
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    Annual Review of Astronomy and Astrophysics 35 (1997), S. 557-605 
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    Notes: Abstract Three cases for mixing not present in standard stellar models are presented: Light element depletion in low mass main-sequence stars, deep mixing in massive stars, and deep mixing in low mass giants. The review begins with the mixing indicators and the predictions of standard models. The observational evidence for anomalous mixing is then presented, followed by the physics of mixing outside the standard model. The status of theoretical models that include extra mixing is then examined.
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    Annual Review of Fluid Mechanics 28 (1996), S. 83-128 
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    Topics: Mechanical Engineering, Materials Science, Production Engineering, Mining and Metallurgy, Traffic Engineering, Precision Mechanics , Physics
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    Annual Review of Fluid Mechanics 28 (1996), S. 11-43 
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    Annual Review of Fluid Mechanics 28 (1996), S. 187-213 
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    Annual Review of Fluid Mechanics 28 (1996), S. 215-248 
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    Annual Review of Fluid Mechanics 28 (1996), S. 323-360 
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    Annual Review of Fluid Mechanics 28 (1996), S. 477-539 
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    Annual Review of Fluid Mechanics 29 (1997), S. 515-567 
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    Topics: Mechanical Engineering, Materials Science, Production Engineering, Mining and Metallurgy, Traffic Engineering, Precision Mechanics , Physics
    Notes: Abstract Modern helicopter aerodynamics is challenging because the flow field generated by a helicopter is extremely complicated and difficult to measure, model, and predict; moreover, experiments are expensive and difficult to conduct. In this article we discuss the basic principles of modern helicopter aerodynamics. Many sophisticated experimental and computational techniques have been employed in an effort to predict performance parameters. Of particular interest is the structure of the rotor wake, which is highly three-dimensional and unsteady, and the rotor-blade pressure distribution, which is significantly affected by the strength and position of the wake. We describe the various modern methods of computation and experiment which span the range from vortex techniques to full three-dimensional Navier-Stokes computations, and from classical probe methods to laser velocimetry techniques. Typical results for the structure of the wake and the blade pressure distribution in both hover and forward flight are presented Despite the complexity of the helicopter flow, significant progress has been made within the last ten years and the future will likely bring marked advances.
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    Annual Review of Genetics 30 (1996), S. 405-439 
    ISSN: 0066-4197
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    Topics: Biology
    Notes: Abstract A growing number of cellular regulatory mechanisms are being linked to protein modification by the polypeptide ubiquitin. These include key transitions in the cell cycle, class I antigen processing, signal transduction pathways, and receptor-mediated endocytosis. In most, but not all, of these examples, ubiquitination of a protein leads to its degradation by the 26S proteasome. Following attachment of ubiquitin to a substrate and binding of the ubiquitinated protein to the proteasome, the bound substrate must be unfolded (and eventually deubiquitinated) and translocated through a narrow set of channels that leads to the proteasome interior, where the polypeptide is cleaved into short peptides. Protein ubiquitination and deubiquitination are both mediated by large enzyme families, and the proteasome itself comprises a family of related but functionally distinct particles. This diversity underlies both the high substrate specificity of the ubiquitin system and the variety of regulatory mechanisms that it serves.
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    Annual Review of Genetics 31 (1997), S. 527-546 
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    Notes: Abstract The general goal of genetic studies of learning and memory is to develop and test theories that explain the animal's behavior in neuroanatomical, neurophysiological, cellular, and molecular terms. In this review we describe the role that gene targeting and other transgenic techniques have had in the study of mammalian learning and memory. We focus especially on the hippocampus, a brain structure that is thought to be central to the processing and temporary storage of complex information. We also discuss the main issues that confront this young field, as well as our vision for its future.
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    Annual Review of Genetics 30 (1996), S. 529-556 
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    Notes: Abstract The Hox homeobox gene family plays a pivotal role in regulating patterning and axial morphogenesis in vertebrates. Molecular characterization of the four Hox clusters has shown that they are evolutionarily related with respect to sequence, organization, and expression, suggesting they arose by duplication and divergence. Transgenic analysis has clearly demonstrated the functional roles of individual genes in a broad range of embryonic tissues, and in compound mutants has addressed the issues of cooperativity and redundancy. There is an emerging picture of the cis-regulatory elements underlying Hox expression, and for the 3' members of the clusters there is a considerable degree of conservation between paralogous genes with respect to their functional roles and regulatory control.
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  • 69
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    Annual Review of Genetics 30 (1996), S. 557-578 
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    Notes: Abstract The ciliated protozoa divide the labor of germline and somatic genetic functions between two distinct nuclei. The development of the somatic (macro-) nucleus from the germinal (micro-) nucleus occurs during sexual reproduction and involves large-scale, genetic reorganization including site-specific chromosome breakage and DNA deletion. This intriguing process has been extensively studied in Tetrahymena thermophila. Characterization of cis-acting sequences, putative protein factors, and possible reaction intermediates has begun to shed light on the underlying mechanisms of genome rearrangement. This article summarizes the current understanding of this phenomenon and discusses its origin and biological function. We postulate that ciliate nuclear restructuring serves to segregate the two essential functions of chromosomes: the transmission and expression of genetic information.
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  • 70
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    Annual Review of Genetics 31 (1997), S. 33-60 
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    Notes: Abstract Production of red blood cells (erythropoiesis) in the vertebrate embryo is critical to its survival and subsequent development. As red cells are the first blood cells to appear in embryogenesis, their origin reflects commitment of mesoderm to an hematopoietic fate and provides an avenue by which to examine the development of the hematopoietic system, including the hematopoietic stem cell (HSC). We discuss the genetics of erythropoiesis as studied in two systems: the mouse and zebrafish (Danio rerio). In the mouse, targeted disruption has established several genes as essential at different stages of hematopoiesis or erythroid precursor cell maturation. In the zebrafish, numerous mutants displaying a wide range of phenotypes have been isolated, although the affected genes are unknown. In comparing mouse knockout and zebrafish mutant phenotypes, we propose a pathway for erythropoiesis that emphasizes the apparent similarity of the mutants and the complementary nature of investigation in the two species. We speculate that further genetic studies in mouse and zebrafish will identify the majority of essential genes and define a regulatory network for hematopoiesis in vertebrates.
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  • 71
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    Annual Review of Genetics 31 (1997), S. 61-89 
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    Notes: Abstract During this decade, there have been major advancements in the understanding of genetic loci involved in synthesis of the family of Mg-tetrapyrroles known as chlorophylls and bacteriochlorophylls. Molecular genetic analysis of Mg-tetrapyrrole biosynthesis was initiated by the performance of detailed sequence and mutational analysis of the photosynthesis gene cluster from Rhodobacter capsulatus. These studies provided the first detailed understanding of genes involved in bacteriochlorophyll a biosynthesis. In the short time since these studies were initiated, most of the chlorophyll biosynthesis genes have been identified by virtue of their ability to complement bacteriochlorophyll a biosynthesis mutants as well as by sequence homology comparisons. This review is centered on a discussion of our current understanding of bacterial, algal, and plant genes that code for enzymes in the Mg-branch of the tetrapyrrole biosynthetic pathway that are responsible for synthesis of chlorophylls and bacteriochlorophylls.
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  • 72
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    Annual Review of Genetics 31 (1997), S. 91-111 
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    Notes: Abstract Gene amplification is a common feature of the genome of prokaryotic organisms. In this review, we analyze different instances of gene amplification in a variety of prokaryotes, including their mechanisms of generation and biological role. Growing evidence supports the concept that gene amplification be considered not as a mutation but rather as a dynamic genomic state related to the adaptation of bacterial populations to changing environmental conditions or biological interactions. In this context, the potentially amplifiable DNA regions impose a defined dynamic structure on the genome. If such structure has indeed been selected during evolution, it is a particularly challenging hypothesis.
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    Annual Review of Biophysics and Biomolecular Structure 25 (1996), S. 1-28 
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    Annual Review of Biophysics and Biomolecular Structure 25 (1996), S. 29-53 
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    Annual Review of Biophysics and Biomolecular Structure 25 (1996), S. 79-112 
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    Annual Review of Biophysics and Biomolecular Structure 25 (1996), S. 137-162 
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    Annual Review of Biophysics and Biomolecular Structure 25 (1996), S. 343-365 
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 401-424 
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    Notes: Abstract Phage display makes large-peptide diversity libraries readily attainable for identifying novel peptide ligands for receptors and other protein or non-protein targets. This technology kindles enthusiasm for the idea that large and protein-protein interaction surfaces (epitopes) can be distilled down to small pharmacophores. These may be accessible to organic scaffolding, yielding new orally active drugs that might otherwise have taken greater time and effort to be discovered through chemical-library screening. This review, though not comprehensive with respect to the explosive volume of phage display work over the last few years, focuses on recent developments in phage-displayed peptide technology.
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 425-459 
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    Notes: Abstract Oil-water partitioning, solubilities, and vapor pressure experiments on small-molecule compounds are often used as models to obtain energies for biomolecular modeling. For example, measured partition coefficients, K, are often inserted into the formula -RTlnK to obtain quantities thought to represent microscopic contact interaction free energies. We review evidence here that this procedure does not always give microscopically meaningful free energies. Some partitioning processes, particularly involving polymeric solvents such as octanol or hexadecane, are governed not only by translational entropies and contact interactions, but also by free energies resulting from changes in the conformations of the polymer chains upon solute insertion. The Flory-Huggins theory is more suitable for these situations than is the classical approach. We discuss the physical bases for both approaches.
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  • 80
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 461-493 
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    Notes: Abstract Ten years have passed since the initial reports that antibodies could be programmed to have enzymatic activity by immunization with a transition-site analog. Much of the research over the last decade has focused on defining the scope and generality of antibody catalysis; however, during the past two years the first few crystal structures of catalytic antibody transition-state analogs have been reported. This review analyzes four such structures of catalytic antibodies that catalyze markedly different reactions, including ester hydrolysis, sulfide oxidation, and a pericyclic rearrangement. Structure-function relations for these catalysts are discussed and compared to the structure and function of natural enzymes, as well as the chemistry that occurs in solution.
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 567-596 
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    Notes: Abstract Recent advances in ultrasensitive instrumentation have allowed for the detection, identification, and dynamic studies of single molecules in the condensed phase. This measurement capability provides a new set of tools for scientists to address important current problems and to explore new frontiers in many scientific disciplines, such as chemistry, molecular biology, molecular medicine, and nanostructured materials. This review focuses on the methodologies and biological applications of single-molecule detection based on laser-induced fluorescence.
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    Annual Review of Biophysics and Biomolecular Structure 26 (1997), S. 629-658 
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    Notes: Abstract This chapter reviews the dynamics information obtained from experimental magnetic resonance studies of site-specifically labeled duplex DNA. A previous review (43) discusses the dynamics of duplex DNA; it develops a theory that shows how magnetic resonance experiments are used to detect those dynamics. The methods for obtaining information about dynamics as well as a summary of what is now known about the site-specific dynamics of DNA are presented. This review contains two methods sections which present results using electron paramagnetic resonance and nuclear magnetic resonance active probes.
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    Annual Review of Cell and Developmental Biology 12 (1996), S. 27-54 
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    Notes: Abstract Each organelle of the secretory pathway is required to selectively allow transit of newly synthesized secretory and plasma membrane proteins and also to maintain a unique set of resident proteins that define its structural and functional properties. In the case of the endoplasmic reticulum (ER), residency is achieved in two ways: (a) prevention of residents from entering newly forming transport vesicles and (b) retrieval of those residents that escape. The latter mechanism is directed by discrete retrieval motifs: Soluble proteins have a H/KDEL sequence at their carboxy-terminus; membrane proteins have a dibasic motif, either di-lysine or di-arginine, located close to the terminus of their cytoplasmic domain. Recently it was found that di-lysine motifs bind the complex of cytosolic coat proteins, COP I, and that this interaction functions in the retrieval of proteins from the Golgi to the ER. Also discussed are the potential roles this interaction may have in vesicular trafficking.
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    Annual Review of Cell and Developmental Biology 12 (1996), S. 91-128 
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    Notes: Abstract The cytokine receptor superfamily is characterized by structural motifs in the exoplasmic domain and by the absence of catalytic activity in the cytosolic segment. Activated by ligand-triggered multimerization, these receptors in turn activate a number of cytosolic signal transduction proteins, including protein tyrosine kinases and phosphatases, and affect an array of cellular functions that include proliferation and differentiation. Molecular study of these receptors is revealing the roles they play in the control of normal hematopoiesis and in the development of disease.
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    Annual Review of Cell and Developmental Biology 12 (1996), S. 221-255 
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    Notes: Abstract A taxonomically diverse group of bacterial pathogens have evolved a variety of strategies to subvert host-cellular functions to their advantage. This often involves two-way biochemical interactions leading to responses in both the pathogen and host cell. Central to this interaction is the function of a specialized protein secretion system that directs the export and/or translocation into the host cells of a number of bacterial proteins that can induce or interfere with host-cell signal transduction pathways. The understanding of these bacterial/host-cell interactions will not only lead to novel therapeutic approaches but will also result in a better understanding of a variety of basic aspects of cell physiology and immunology.
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    Annual Review of Cell and Developmental Biology 12 (1996), S. 305-333 
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    Notes: Abstract In this chapter, we review the structure and composition of interphase and mitotic chromosomes. We discuss how these observations support the model that mitotic condensation is a deterministic process leading to the invariant folding of a given chromosome. The structural studies have also placed constraints on the mechanism of condensation and defined several activities needed to mediate condensation. In the context of these activities and structural information, we present our current understanding of the role of cis sites, histones, topoisomerase II, and SMC proteins in condensation. We conclude by using our current knowledge of mitotic condensation to address the differences in chromosome condensation observed from bacteria to humans and to explore the relevance of this process to other processes such as gene expression.
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    Annual Review of Cell and Developmental Biology 12 (1996), S. 463-519 
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    Notes: Abstract Focal adhesions are sites of tight adhesion to the underlying extracellular matrix developed by cells in culture. They provide a structural link between the actin cytoskeleton and the extracellular matrix and are regions of signal transduction that relate to growth control. The assembly of focal adhesions is regulated by the GTP-binding protein Rho. Rho stimulates contractility which, in cells that are tightly adherent to the substrate, generates isometric tension. In turn, this leads to the bundling of actin filaments and the aggregation of integrins (extracellular matrix receptors) in the plane of the membrane. The aggregation of integrins activates the focal adhesion kinase and leads to the assembly of a multicomponent signaling complex.
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    Annual Review of Cell and Developmental Biology 12 (1996), S. 543-573 
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    Notes: Abstract Motor proteins perform a wide variety of functions in all eukaryotic cells. Recent advances in the structural and mutagenic analysis of the myosin motor has led to insights into how these motors transduce chemical energy into mechanical work. This review focuses on the analysis of the effects of myosin mutations from a variety of organisms on the in vivo and in vitro properties of this ubiquitous motor and illustrates the positions of these mutations on the high-resolution three-dimensional structure of the myosin motor domain.
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    Annual Review of Cell and Developmental Biology 13 (1997), S. 203-229 
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    Notes: Abstract To grow and develop optimally, all organisms need to perceive and process information from both their biotic and abiotic surroundings. A particularly important environmental cue is light, to which organisms respond in many different ways. Because they are photosynthetic and non-motile, plants need to be especially plastic in response to their light environment. The diverse responses of plants to light require sophisticated sensing of its intensity, direction, duration, and wavelength. The action spectra of light responses provided assays to identify three photoreceptor systems absorbing in the red/far-red, blue/near-ultraviolet, and ultraviolet spectral ranges. Following absorption of light, photoreceptors interact with other signal transduction elements, which eventually leads to many molecular and morphological responses. While a complete signal transduction cascade is not known yet, molecular genetic studies using the model plant Arabidopsis have led to substantial progress in dissecting the signal transduction network. Important gains have been made in determining the function of the photoreceptors, the terminal response pathways, and the intervening signal transduction components.
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    Annual Review of Cell and Developmental Biology 13 (1997), S. 231-259 
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    Notes: Abstract Adipose tissue has long been known to house the largest energy reserves in the animal body. Recent research indicates that in addition to this role, the adipocyte functions as a global regulator of energy metabolism. Adipose tissue is exquisitely sensitive to a variety of endocrine and paracrine signals, e.g. insulin, glucagon, glucocorticoids, and tumor necrosis factor (TNF), that combine to control both the secretion of other regulatory factors and the recruitment and differentiation of new adipocytes. The process of adipocyte differentiation is controlled by a cascade of transcription factors, most notably those of the C/EBP and PPAR families, which combine to regulate each other and to control the expression of adipocyte-specific genes. One such gene, i.e. the obese gene, was recently identified and found to encode a hormone, referred to as leptin, that plays a major role in the regulation of energy intake and expenditure. The hormonal and transcriptional control of adipocyte differentiation is discussed, as is the role of leptin and other factors secreted by the adipocyte that participate in the regulation of adipose homeostasis.
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    Annual Review of Astronomy and Astrophysics 34 (1996), S. 1-34 
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    Annual Review of Astronomy and Astrophysics 34 (1996), S. 75-109 
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    Notes: Abstract In the past decade a number of observational and theoretical studies have appeared that address the problem of how both the physical conditions in subsurface layers of the Sun and the nature of the magnetic flux tubes of active regions are reflected in the structure and behavior of these regions at the surface. This review discusses work in this area. Many characteristics of plages and sunspot groups are shown to be related to the conditions encountered by the region flux tube as it rises through the convective zone of the Sun to the surface. Size distributions, rotation and meridional flow rates and their covariances, and characteristics of growth and decay are among the factors that have been shown to depend on the nature of the source magnetic flux tube and the physical effects, such as the Coriolis force and magnetic tension, that act deep in the convection zone.
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    Annual Review of Astronomy and Astrophysics 34 (1996), S. 331-381 
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    Annual Review of Astronomy and Astrophysics 34 (1996), S. 419-459 
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    Notes: Abstract The status of searches for gravitational microlensing events of the stars in our galaxy and in other galaxies of the Local Group, the interpretation of the results, some theory, and prospects for the future are reviewed. The searches have already unveiled ~ 100 events, at least two of them caused by binaries, and have already proven to be useful for studies of the Galactic structure. The events detected so far are probably attributable to the effects of ordinary stars, and possibly to substellar brown dwarfs; however, a firm conclusion cannot be reached yet because the analysis published to date is based on a total of only 16 events. The current searches, soon to be upgraded, will probably allow determination of the mass function of stars and brown dwarfs in the next few years; these efforts will also provide good statistical information about binary systems, in particular their mass ratios. They may also reveal the nature of dark matter and allow us to detect planets and planetary mass objects.
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    Annual Review of Astronomy and Astrophysics 34 (1996), S. 461-510 
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    Notes: Abstract A careful assessment of current uncertainties in stellar physics (opacities, nuclear reaction rates, equation of state effects, diffusion, rotation, and mass loss), in the chemistry of globular cluster (GC) stars, and in the cluster distance scale, suggests that the most metal-poor (presumably the oldest) of the Galaxy's GCs have ages near 15 Gyr. Ages below 12 Gyr or above 20 Gyr appear to be highly unlikely. If these = 2 sigma limits are increased by ~ 1 Gyr to account for the formation time of the globulars, and if standard Friedmann cosmologies with the cosmological constant set to zero are assumed, then the GC constraint on the present age of the Universe (t0〉= 13 Gyr) implies that the Hubble constant H0〈= 51 km s-1 Mpc-1 if the density parameter Omega = 1 or 〈= 62 km s-1 Mpc-1 if Omega = 0.3.
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    Annual Review of Astronomy and Astrophysics 34 (1996), S. 241-277 
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    Notes: Abstract The cooling flows or winds from evolved stars are ideal for the formation of molecules and dust. The main location of molecular synthesis is the outer circumstellar envelope, where UV radiation from the interstellar medium penetrates the envelope and, by photodissociating parent molecules, produces the high-energy radicals and ions that activate gas-phase neutral and ion-molecule chemistry. After introducing relevant observational results and theoretical ideas, the salient aspects of the photochemical model are described. The primary application is to the nearby C star, IRC + 10216, where 50 or more circumstellar molecules have been detected. Recent interferometer maps, with resolution approaching 1'', provide the means to verify the main ideas of the model and to indicate directions for its improvement.
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    Annual Review of Astronomy and Astrophysics 34 (1996), S. 703-747 
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    Notes: Abstract Accretion disks are important for many astrophysical phenomena, including galactic nuclei, interacting binary stars, and young stellar objects. The central issue in the theory of accretion disks is to identify the dominant mechanisms that regulate angular momentum transfer and mass flow in a variety of contexts. In the first part of this review, we described some recent advances in the study of the physical processes that may be present in accretion disks. Concurrent with these theoretical developments, the arrival of high-resolution astronomical instruments has led to explosive progress on the observational side. In many cases, the study of accretion disks has evolved from their inferred presence based on circumstantial evidence to direct imaging and detailed spectral analyses. Here, we summarize the theoretical interpretation of these data. We review the constraints that may be imposed on the efficiency and nature of angular momentum transfer processes in a variety of astrophysical contexts.
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    Annual Review of Astronomy and Astrophysics 35 (1997), S. 1-32 
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    Notes: Abstract Eta Carinae (Eta) is one of the most remarkable of all well-studied stars and perhaps the most poorly understood. Observations with the Hubble Space Telescope and other modern instruments have solved a few of the mysteries concerning this object while opening a comparable number of new ones. In this review we first recount some essential background information concerning Eta, then we sketch most of the observational developments of the past few years, related to the star itself and to its ejecta. Throughout, we propose a series of specific unsolved observational and theoretical problems that seem especially interesting or important at this time.
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    Annual Review of Astronomy and Astrophysics 35 (1997), S. 137-177 
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    Notes: Abstract As progressively cooler stellar and substellar objects are discovered, the presence first of molecules and then of condensed particulates greatly complicates the understanding of their physical properties. Accurate model atmospheres that include these processes are the key to establishing their atmospheric parameters. They play a crucial role in determining structural characteristics by setting the surface conditions of model interiors and providing transformations to the various observational planes. They can reveal the spectroscopic properties of brown dwarfs and help establish their detectability. In this paper, we review the current state-of-the-art theory and modeling of the atmospheres of very low mass stars, including the coolest known M dwarfs, M subdwarfs, and brown dwarfs, i.e. Teff〈= 4,000 K and -4.0 〈= [M/H] 〈= +0.0. We discuss ongoing efforts to incorporate molecular and grain opacities in cool stellar spectra, as well as the latest progress in (a) deriving the effective temperature scale of M dwarfs, (b) reproducing the lower main sequences of metal-poor subdwarfs in the halo and globular clusters, and (c) results of the models related to the search for brown dwarfs.
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    Annual Review of Astronomy and Astrophysics 35 (1997), S. 179-215 
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    Source: Annual Reviews Electronic Back Volume Collection 1932-2001ff
    Topics: Physics
    Notes: Abstract All neutral atomic hydrogen gas and a large fraction of the molecular gas in the Milky Way Galaxy and external galaxies lie in PDRs, and PDRs are the origin of most of the nonstellar infrared (IR) and the millimeter CO emission from a galaxy. On the surfaces (Av〈 1-3) of interstellar clouds, the absorption of far ultraviolet (FUV) photons (hnu〈 13.6 eV) by gas and dust grains leads to intense emission of [C II] 158 mum, [O I] 63, 146 mum, and H2 rovibrational transitions, as well as IR dust continuum and polycyclic aromatic hydrocarbon (PAH) emission features. Deeper in PDRs, CO rotational and [C I] 370, 609 mum lines originate. The transition of H to H2 and C+ to CO occurs within PDRs. Theoretical models compared with observations diagnose such physical parameters as the density and temperature structure, the elemental abundances, and the FUV radiation field in PDRs. Applications include clouds next to H II regions, reflection nebulae, planetary nebulae, red giant outflows, circumstellar gas around young stars, diffuse clouds, the warm neutral medium (WNM), and molecular clouds in the interstellar radiation field: in summary, much of the interstellar medium in galaxies. This review focuses on dense PDRs in the Milky Way Galaxy. Theoretical PDR models help explain the observed correlation of the CO J = 1-0 luminosity with the molecular mass and also suggest FUV-induced feedback mechanisms that may regulate star formation rates and the column density through giant molecular clouds.
    Type of Medium: Electronic Resource
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